Abstract

The p53 tumor suppressor gene is a major target for inactivation in human cancer. In non-stressed normal cells, the p53 protein is practically latent, owing to its being present in very low amounts and in a rather inactive molecular form. The relative lack of activity of p53 under such conditions is largely due to the action of Mdm2, which targets p53 for rapid degradation and, furthermore, maintains p53 in a complex that is incompatible with efficient performance of p53 as a transcription factor. In response to a variety of stress signals, particularly those that are closely linked with cancer (e.g. genomic damage, oncogene activation), p53 is freed of the inhibitory effects of Mdm2. This results in stabilization and activation of p53, leading to a multitude of biochemical and biological effects. The consequence of such p53 activation, when occurring in an incipient cancer cell, is the elimination of such cell from the replicative pool, preventing its further progression into a life-threatening tumor. The long term objective of this project is to elucidate the mechanisms responsible for maintaining p53 inactive in non-stressed cells, the biochemical events that enable p53 activation in response to cancer-related stress, and the molecular basis for the failure of p53 to function properly in human cancer cells, even when retained in its wild type form. Specifically, this work will address the impact of covalent modifications on Mdm2, particularly acetylation, evaluate the exact nature of the changes that are imposed on p53 as a consequence of Mdm2 activity, investigate the idea that some of the inhibitory effects of Mdm2 may involve its interaction with the chromatin of p53 target genes in a manner leading to transcriptional silencing, explore the possibility that dominant negative forms of p63, a p53 family member, are responsible for the failure of p53 to function as an effective tumor suppressor in some human cancers, and elucidate the regulation of p53 activation by cell-cell interaction and its relevance for the conversion of epithelial tumors to a more malignant state. The methodology will include a combination of cell-free assays for protein activity, mutational analysis and genetic manipulation of cultured cells, analysis of protein-protein interactions, gene expression analysis, and in vivo experiments in normal and cancer-bearing mice. Success of the proposed experiments should allow a better understanding of the regulation of p53 activity and its subversion in cancer, and provide clues for improved cancer therapy.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Cancer Institute (NCI)
Type
Method to Extend Research in Time (MERIT) Award (R37)
Project #
5R37CA040099-28
Application #
8278422
Study Section
Special Emphasis Panel (NSS)
Program Officer
Watson, Joanna M
Project Start
1985-08-15
Project End
2013-07-30
Budget Start
2012-08-01
Budget End
2013-07-30
Support Year
28
Fiscal Year
2012
Total Cost
$219,151
Indirect Cost
$16,233

  Institution

Name
Weizmann Institute of Science
Department
Type
DUNS #
600048466
City
Rehovot, Israel
State
Country
Israel
Zip Code
76100

  Publications

Tarcic, Ohad; Pateras, Ioannis S; Cooks, Tomer et al. (2016) RNF20 Links Histone H2B Ubiquitylation with Inflammation and Inflammation-Associated Cancer. Cell Rep 14:1462-1476
Levine, Benjamin D; Cagan, Ross L (2016) Drosophila Lung Cancer Models Identify Trametinib plus Statin as Candidate Therapeutic. Cell Rep 14:1477-1487
Aylon, Y; Sarver, A; Tovy, A et al. (2014) Lats2 is critical for the pluripotency and proper differentiation of stem cells. Cell Death Differ 21:624-33
Hoffman, Yonit; Pilpel, Yitzhak; Oren, Moshe (2014) microRNAs and Alu elements in the p53-Mdm2-Mdm4 regulatory network. J Mol Cell Biol 6:192-7
Hoffman, Y; Bublik, D R; Pilpel, Y et al. (2014) miR-661 downregulates both Mdm2 and Mdm4 to activate p53. Cell Death Differ 21:302-9
Cooks, Tomer; Harris, Curtis C; Oren, Moshe (2014) Caught in the cross fire: p53 in inflammation. Carcinogenesis 35:1680-90
Cooks, Tomer; Pateras, Ioannis S; Tarcic, Ohad et al. (2013) Mutant p53 prolongs NF-?B activation and promotes chronic inflammation and inflammation-associated colorectal cancer. Cancer Cell 23:634-46
Shema-Yaacoby, Efrat; Nikolov, Miroslav; Haj-Yahya, Mahmood et al. (2013) Systematic identification of proteins binding to chromatin-embedded ubiquitylated H2B reveals recruitment of SWI/SNF to regulate transcription. Cell Rep 4:601-8
Golomb, Lior; Bublik, Debora Rosa; Wilder, Sylvia et al. (2012) Importin 7 and exportin 1 link c-Myc and p53 to regulation of ribosomal biogenesis. Mol Cell 45:222-32
Fuchs, Gilad; Shema, Efrat; Vesterman, Rita et al. (2012) RNF20 and USP44 regulate stem cell differentiation by modulating H2B monoubiquitylation. Mol Cell 46:662-73

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